Delivery of PEGylated liposomal doxorubicin by bispecific antibodies improves treatment in models of high-risk childhood leukemia

Author:

Moles Ernest123ORCID,Howard Christopher B.4ORCID,Huda Pie4ORCID,Karsa Mawar13ORCID,McCalmont Hannah13ORCID,Kimpton Kathleen13ORCID,Duly Alastair13ORCID,Chen Yongjuan13ORCID,Huang Yizhou13ORCID,Tursky Melinda L.567ORCID,Ma David567,Bustamante Sonia8ORCID,Pickford Russell8ORCID,Connerty Patrick13ORCID,Omari Sofia13ORCID,Jolly Christopher J.9ORCID,Joshi Swapna9,Shen Sylvie9,Pimanda John E.3910ORCID,Dolnikov Alla13,Cheung Laurence C.1112ORCID,Kotecha Rishi S.11121314ORCID,Norris Murray D.1315ORCID,Haber Michelle13ORCID,de Bock Charles E.13ORCID,Somers Klaartje13ORCID,Lock Richard B.13,Thurecht Kristofer J.416ORCID,Kavallaris Maria123ORCID

Affiliation:

1. Children’s Cancer Institute, Lowy Cancer Research Centre, UNSW Sydney, Sydney 2052, Australia.

2. Australian Centre for Nanomedicine, Faculty of Engineering, UNSW Sydney, Sydney 2052, Australia.

3. School of Clinical Medicine, Medicine and Health, UNSW Sydney, Sydney 2052, Australia.

4. Australian Institute for Bioengineering and Nanotechnology, University of Queensland, St Lucia 4072, Australia.

5. Department of Haematology and Bone Marrow Transplant, St Vincent's Hospital Sydney, Sydney 2010, Australia.

6. St Vincent's Centre for Applied Medical Research (AMR), Sydney 2010, Australia.

7. St Vincent Clinical School, Faculty of Medicine and Health, UNSW Sydney, Sydney 2052, Australia.

8. Bioanalytical Mass Spectrometry Facility, Mark Wainwright Analytical Centre, UNSW Sydney, Sydney 2052, Australia.

9. School of Biomedical Sciences, Lowy Cancer Research Centre, UNSW Sydney, Sydney 2052, Australia.

10. Department of Haematology, Prince of Wales Hospital, Sydney 2031, Australia.

11. Leukaemia Translational Research Laboratory, Telethon Kids Cancer Centre, Telethon Kids Institute, Perth, Western Australia 6009, Australia.

12. Curtin Medical School, Curtin University, Perth, Western Australia 6102, Australia.

13. Department of Clinical Haematology, Oncology, Blood and Marrow Transplantation, Perth Children’s Hospital, Perth, Western Australia 6009, Australia.

14. School of Medicine, University of Western Australia, Perth, Western Australia 6009, Australia.

15. University of New South Wales Centre for Childhood Cancer Research, UNSW Sydney, Sydney 2052, Australia.

16. Centre for Advanced Imaging, ARC Training Centre for Innovation in Biomedical Imaging Technologies, University of Queensland, St Lucia 4072, Australia.

Abstract

High-risk childhood leukemia has a poor prognosis because of treatment failure and toxic side effects of therapy. Drug encapsulation into liposomal nanocarriers has shown clinical success at improving biodistribution and tolerability of chemotherapy. However, enhancements in drug efficacy have been limited because of a lack of selectivity of the liposomal formulations for the cancer cells. Here, we report on the generation of bispecific antibodies (BsAbs) with dual binding to a leukemic cell receptor, such as CD19, CD20, CD22, or CD38, and methoxy polyethylene glycol (PEG) for the targeted delivery of PEGylated liposomal drugs to leukemia cells. This liposome targeting system follows a “mix-and-match” principle where BsAbs were selected on the specific receptors expressed on leukemia cells. BsAbs improved the targeting and cytotoxic activity of a clinically approved and low-toxic PEGylated liposomal formulation of doxorubicin (Caelyx) toward leukemia cell lines and patient-derived samples that are immunophenotypically heterogeneous and representative of high-risk subtypes of childhood leukemia. BsAb-assisted improvements in leukemia cell targeting and cytotoxic potency of Caelyx correlated with receptor expression and were minimally detrimental in vitro and in vivo toward expansion and functionality of normal peripheral blood mononuclear cells and hematopoietic progenitors. Targeted delivery of Caelyx using BsAbs further enhanced leukemia suppression while reducing drug accumulation in the heart and kidneys and extended overall survival in patient-derived xenograft models of high-risk childhood leukemia. Our methodology using BsAbs therefore represents an attractive targeting platform to potentiate the therapeutic efficacy and safety of liposomal drugs for improved treatment of high-risk leukemia.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

General Medicine

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